Bloqueio da integrina αvβ3 inibe apoptose e induz autofagia em células tumorais de cancêr de mama

Detalhes bibliográficos
Autor(a) principal: Lino, Rafael Luis Bressani
Data de Publicação: 2018
Tipo de documento: Dissertação
Idioma: por
Título da fonte: Repositório Institucional da UFSCAR
Texto Completo: https://repositorio.ufscar.br/handle/ufscar/10880
Resumo: Integrins are key receptors that mediate cell adhesion to the extracellular matrix (ECM) and regulate cell behavior including cell migration. Particularly, αvβ3 integrin, the vitronectin receptor, plays a key role in both physiological angiogenesis and in tumor progression. This receptor recognizes the arginine-glycine-aspartic acid (RGD) motif in ECM proteins and it can be antagonized by RGD-peptides, resulting in decreased cell migration and invasion. RGD-based drugs have shown disappointing results in clinical trials; however, the reasons for their lack of activity are still obscure. Aiming to contribute to a better understanding on the molecular consequences of integrin inhibition, we have tested a recombinant RGD-disintegrin (DisBa-01) in two types of murine cell lines, breast tumor 4T1BM2 cells and L929 fibroblasts. Only tumor cells showed decreased motility and adhesion as well as morphologic alterations upon DisBa-01 treatment. This result was attributed to the higher levels of αvβ3 in 4T1BM2 cells making them more sensitive to DisBa-01 blocking. Flow cytometry analysis showed that DisBa-01 induced cell cycle arrest at S phase in 4T1BM2 cells, but did not induce apoptosis, which was consistent with the decrease in caspase-3, 8 and 9 expression at mRNA and protein levels. It was also observed that this disintegrin increases LC3B expression in both cell lines, an indicator of autophagic induction. In conclusion, DisBa-01 specificity towards 4T1BM2 cells when compared to L929, could be due to the higher level of expression of αv and β3 integrins in these cells, and these observations suggest new insights on the effects of RGD-based inhibitors considering their importance on drug development for human health.
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spelling Lino, Rafael Luis BressaniAraújo, Heloísa Sobreiro Selistre dehttp://lattes.cnpq.br/4065824911933203http://lattes.cnpq.br/9514190453774618455de91f-ec32-49aa-ae80-74de2c3eb49e2019-01-30T10:44:19Z2019-01-30T10:44:19Z2018-12-17LINO, Rafael Luis Bressani. Bloqueio da integrina αvβ3 inibe apoptose e induz autofagia em células tumorais de cancêr de mama. 2018. Dissertação (Mestrado em Ciências Fisiológicas) – Universidade Federal de São Carlos, São Carlos, 2018. Disponível em: https://repositorio.ufscar.br/handle/ufscar/10880.https://repositorio.ufscar.br/handle/ufscar/10880Integrins are key receptors that mediate cell adhesion to the extracellular matrix (ECM) and regulate cell behavior including cell migration. Particularly, αvβ3 integrin, the vitronectin receptor, plays a key role in both physiological angiogenesis and in tumor progression. This receptor recognizes the arginine-glycine-aspartic acid (RGD) motif in ECM proteins and it can be antagonized by RGD-peptides, resulting in decreased cell migration and invasion. RGD-based drugs have shown disappointing results in clinical trials; however, the reasons for their lack of activity are still obscure. Aiming to contribute to a better understanding on the molecular consequences of integrin inhibition, we have tested a recombinant RGD-disintegrin (DisBa-01) in two types of murine cell lines, breast tumor 4T1BM2 cells and L929 fibroblasts. Only tumor cells showed decreased motility and adhesion as well as morphologic alterations upon DisBa-01 treatment. This result was attributed to the higher levels of αvβ3 in 4T1BM2 cells making them more sensitive to DisBa-01 blocking. Flow cytometry analysis showed that DisBa-01 induced cell cycle arrest at S phase in 4T1BM2 cells, but did not induce apoptosis, which was consistent with the decrease in caspase-3, 8 and 9 expression at mRNA and protein levels. It was also observed that this disintegrin increases LC3B expression in both cell lines, an indicator of autophagic induction. In conclusion, DisBa-01 specificity towards 4T1BM2 cells when compared to L929, could be due to the higher level of expression of αv and β3 integrins in these cells, and these observations suggest new insights on the effects of RGD-based inhibitors considering their importance on drug development for human health.As integrinas são receptores-chave que regulam a adesão celular à matriz extracelular (ECM), além de modularem o comportamento e a migração das células. Particularmente, a integrina αvβ3, receptor de vitronectina, desempenha um papel fundamental tanto na angiogênese fisiológica quanto na progressão tumoral. Este receptor reconhece o motivo arginina-glicina-ácido aspártico (RGD) nas proteínas da MEC e pode ser antagonizado pelos peptídeos RGD, resultando na diminuição da migração e da invasão celular. Fármacos baseadas no motivo RGD mostraram resultados não promissores em ensaios clínicos, no entanto, as razões para sua falta de atividade ainda permanecem desconhecidas. Para uma melhor compreensão dos mecanismos moleculares da inibição de integrinas, testamos uma desintegrina RGD recombinante (DisBa-01) em dois tipos de linhagens celulares: 4T1BM2 de tumor de mama murino e fibroblastos L929. Apenas as células tumorais apresentaram diminuição da motilidade e da adesão celular, bem como alterações morfológicas após tratamento com DisBa-01. Estes resultados foram atribuídos aos níveis mais altos de αvβ3 nas células 4T1BM2, tornando-as mais sensíveis ao bloqueio feito pela desintegrina. A análise por citometria de fluxo mostrou que DisBa-01 induziu parada do ciclo celular na fase S em células 4T1BM2, mas não induziu apoptose, o que foi condizente com a diminuição da expressão gênica de caspase-3, 8 e 9. A presença de caspase-3 ativa não foi detectada por Western Blotting em ambas as células. Em contrapartida, foi observado que DisBa-01 aumenta a expressão proteica de LC3B, um indicador de autofagia. Em conclusão, a especificidade de DisBa-01 em relação às células 4T1BM2 quando comparada às células L929, pode ser devido ao maior nível de expressão de integrinas αv e β3 nas células tumorais. Estas observações sugerem novos mecanismos sobre os efeitos de inibidores baseados em RGD, considerando sua importância terapêutica para a saúde humana.Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq)Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES)CNPq: 132271/2016-8porUniversidade Federal de São CarlosCâmpus São CarlosPrograma Interinstitucional de Pós-Graduação em Ciências Fisiológicas - PIPGCFUFSCarCâncer de mamaIntegrina αvβ3MMP-2Adesão celularAnoikisApoptoseAutofagiaDesintegrinas-RGDCIENCIAS BIOLOGICAS::FISIOLOGIABloqueio da integrina αvβ3 inibe apoptose e induz autofagia em células tumorais de cancêr de mamaBlocking αvβ3 inhibits apoptosis by inducing autophagy in murine breast tumor cellsinfo:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/masterThesis6 meses após a data da defesa600600b61211db-d955-45b7-886e-a0cefb89980finfo:eu-repo/semantics/openAccessreponame:Repositório Institucional da UFSCARinstname:Universidade Federal de São Carlos (UFSCAR)instacron:UFSCARORIGINALDissertação de Mestrado - Rafael L. 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dc.title.por.fl_str_mv Bloqueio da integrina αvβ3 inibe apoptose e induz autofagia em células tumorais de cancêr de mama
dc.title.alternative.eng.fl_str_mv Blocking αvβ3 inhibits apoptosis by inducing autophagy in murine breast tumor cells
title Bloqueio da integrina αvβ3 inibe apoptose e induz autofagia em células tumorais de cancêr de mama
spellingShingle Bloqueio da integrina αvβ3 inibe apoptose e induz autofagia em células tumorais de cancêr de mama
Lino, Rafael Luis Bressani
Câncer de mama
Integrina αvβ3
MMP-2
Adesão celular
Anoikis
Apoptose
Autofagia
Desintegrinas-RGD
CIENCIAS BIOLOGICAS::FISIOLOGIA
title_short Bloqueio da integrina αvβ3 inibe apoptose e induz autofagia em células tumorais de cancêr de mama
title_full Bloqueio da integrina αvβ3 inibe apoptose e induz autofagia em células tumorais de cancêr de mama
title_fullStr Bloqueio da integrina αvβ3 inibe apoptose e induz autofagia em células tumorais de cancêr de mama
title_full_unstemmed Bloqueio da integrina αvβ3 inibe apoptose e induz autofagia em células tumorais de cancêr de mama
title_sort Bloqueio da integrina αvβ3 inibe apoptose e induz autofagia em células tumorais de cancêr de mama
author Lino, Rafael Luis Bressani
author_facet Lino, Rafael Luis Bressani
author_role author
dc.contributor.authorlattes.por.fl_str_mv http://lattes.cnpq.br/9514190453774618
dc.contributor.author.fl_str_mv Lino, Rafael Luis Bressani
dc.contributor.advisor1.fl_str_mv Araújo, Heloísa Sobreiro Selistre de
dc.contributor.advisor1Lattes.fl_str_mv http://lattes.cnpq.br/4065824911933203
dc.contributor.authorID.fl_str_mv 455de91f-ec32-49aa-ae80-74de2c3eb49e
contributor_str_mv Araújo, Heloísa Sobreiro Selistre de
dc.subject.por.fl_str_mv Câncer de mama
Integrina αvβ3
MMP-2
Adesão celular
Anoikis
Apoptose
Autofagia
Desintegrinas-RGD
topic Câncer de mama
Integrina αvβ3
MMP-2
Adesão celular
Anoikis
Apoptose
Autofagia
Desintegrinas-RGD
CIENCIAS BIOLOGICAS::FISIOLOGIA
dc.subject.cnpq.fl_str_mv CIENCIAS BIOLOGICAS::FISIOLOGIA
description Integrins are key receptors that mediate cell adhesion to the extracellular matrix (ECM) and regulate cell behavior including cell migration. Particularly, αvβ3 integrin, the vitronectin receptor, plays a key role in both physiological angiogenesis and in tumor progression. This receptor recognizes the arginine-glycine-aspartic acid (RGD) motif in ECM proteins and it can be antagonized by RGD-peptides, resulting in decreased cell migration and invasion. RGD-based drugs have shown disappointing results in clinical trials; however, the reasons for their lack of activity are still obscure. Aiming to contribute to a better understanding on the molecular consequences of integrin inhibition, we have tested a recombinant RGD-disintegrin (DisBa-01) in two types of murine cell lines, breast tumor 4T1BM2 cells and L929 fibroblasts. Only tumor cells showed decreased motility and adhesion as well as morphologic alterations upon DisBa-01 treatment. This result was attributed to the higher levels of αvβ3 in 4T1BM2 cells making them more sensitive to DisBa-01 blocking. Flow cytometry analysis showed that DisBa-01 induced cell cycle arrest at S phase in 4T1BM2 cells, but did not induce apoptosis, which was consistent with the decrease in caspase-3, 8 and 9 expression at mRNA and protein levels. It was also observed that this disintegrin increases LC3B expression in both cell lines, an indicator of autophagic induction. In conclusion, DisBa-01 specificity towards 4T1BM2 cells when compared to L929, could be due to the higher level of expression of αv and β3 integrins in these cells, and these observations suggest new insights on the effects of RGD-based inhibitors considering their importance on drug development for human health.
publishDate 2018
dc.date.issued.fl_str_mv 2018-12-17
dc.date.accessioned.fl_str_mv 2019-01-30T10:44:19Z
dc.date.available.fl_str_mv 2019-01-30T10:44:19Z
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
dc.type.driver.fl_str_mv info:eu-repo/semantics/masterThesis
format masterThesis
status_str publishedVersion
dc.identifier.citation.fl_str_mv LINO, Rafael Luis Bressani. Bloqueio da integrina αvβ3 inibe apoptose e induz autofagia em células tumorais de cancêr de mama. 2018. Dissertação (Mestrado em Ciências Fisiológicas) – Universidade Federal de São Carlos, São Carlos, 2018. Disponível em: https://repositorio.ufscar.br/handle/ufscar/10880.
dc.identifier.uri.fl_str_mv https://repositorio.ufscar.br/handle/ufscar/10880
identifier_str_mv LINO, Rafael Luis Bressani. Bloqueio da integrina αvβ3 inibe apoptose e induz autofagia em células tumorais de cancêr de mama. 2018. Dissertação (Mestrado em Ciências Fisiológicas) – Universidade Federal de São Carlos, São Carlos, 2018. Disponível em: https://repositorio.ufscar.br/handle/ufscar/10880.
url https://repositorio.ufscar.br/handle/ufscar/10880
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dc.publisher.none.fl_str_mv Universidade Federal de São Carlos
Câmpus São Carlos
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dc.publisher.initials.fl_str_mv UFSCar
publisher.none.fl_str_mv Universidade Federal de São Carlos
Câmpus São Carlos
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